DNA-Seq

Strand NGS supports an extensive workflow for the analysis and visualization of DNA-Seq data – such as from whole genome, whole exome or targeted resequencing experiments. The workflow includes the ability to detect variants (SNPs, MNPs and short InDels), annotate them with dbSNP, and identify the effect on transcripts of non-synonymous coding SNPs. Further downstream analysis such as GO, pathway analysis, etc can be performed on the set of affected genes. Large structural variations, including large insertions, deletions, inversions, and translocations, can also be detected with paired-end or mate-paired data. In addition, copy number variations can be detected using tumor-normal pairs.

Variant Support View

View the delta-neighbourhood of SNPs in high coverage locations. Collapse reads into clusters to quickly verify predicted SNPs. Color with base quality or mapping quality, and annotate with strand information for more insight.

SNP Effect Analysis

Predict the effect of SNPs on the provided transcript annotations and identify SNPs of interest. Link out to dbSNP for more details.

Structural Variant Analysis

Detect structural variants in paired end data and identify large structural variants, including large deletions, insertions, inversions, and translocations. In addition, detect structural variants using split reads.

Manipulate Region Lists

One-Shot Pipeline

Execute one-shot pipeline for quick analysis and compute-intensive tasks using the Pipeline Manager. Also, configure pipelines or import customized pipelines using a .json file to perform reiterative tasks. Pipeline Manager also allows interaction with the user interface even as the pipelines are being executed in the background.

GO Analysis

Perform GO analysis on the set of genes affected by identified variants.

Pathway Analysis

Use the packaged Interaction Database of over 2 million interactions (with supporting PubMed references) or other curated pathways to find relationships between genes. Learn more

Compare gene lists

Compare different gene lists from multiple experiments and across organisms.